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I am not sure what your experience is with your neuro, but most of us were handed a bag of literature and tapes and told to go home and call back when we chose a drug. I don't know of any other disease where they do that. Many folks are on one or another of the "CRABs" For some, their choice works very well. For others, they run through all of the choices. Obviously, on this Tysabri thread, there are people who Tysabri is working for, so we can be called "Tysabri cheerleaders" There are also a lot of folks who have been here who, for one reason or another, have chosen to stop Tysabri and moved on to another therapy, or chosen to go "naked" and not choose anything for now. One of our objectives when we fought to get Tysabri returned to market was to allow us the opportunity to make an informed decision and choose the drug we wanted. This board exists to support people and give them all the information we have to help them make an informed choice. They can talk to people who are on each of the drugs and assess the risks involved for each of them, the ease of use, the side effects, and hear others' stories on the good and the bad. Each time a new report of PML comes out, folks who are on Tysabri each have to make the decision all over again in their head, to continue taking Tysabri or to make another choice. Regardless of what anyone's personal choice is, we support them in their decision. I for one, have chosen to stay on Tysabri once again, after the latest case of PML that was reported, with the information I have received here and from other sources. Let us know how you are doing and we will support you in whatever therapy you choose! :hug: |
Thanks to Komokazi for the heads up!
Info on the 10th PML case is now on Elan's site. In brief: On 23 June 2009, tenth confirmed post-marketing diagnosis of PML in a 27 year old male in the EU with a history of MS. The patient had previous exposure to interferon-beta, Copaxone, and IVIG. The patient received 30 TYSABRI doses between January 2007 and June 2009. Symptoms began with right hand weakness. MRI scans revealed new lesions in the left motor and parietal cortex. PCR of CSF returned 250-500 copies of JCV. Plasma exchanged started. Patient is reported to be stable according to treating physician. More good info: PML lesions do NOT enhance with contrast on MRI. I think I knew that but forgot it, and I may have posted it before. I just woke up and haven't finished coffee quart #1 yet! |
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It's exciting to hear of people that are good responders to any drug, really.... a lot of times you just hear the stories of people who the med works only so-so for them, or not at all, which is unfortunate. It's reassuring that I have come across a few good positive stories for the ABCR/CRAB drugs (where the heck does that second acronym come from btw?) A question on PML-- is it fair to say that this is a disease that comes about as a result of immune suppression or is the reason not very well understood yet? Also, a question on Tysabri-- does it impair one's immune function in a general way, or is it more targeted to the MS? In other words, does one have a higher risk of coming down with common viruses/bacterial infections? And does one tend to stay sick longer? Thanks! |
Hi PL,
I've heard of other people having problems with infections, but I am one of those people who never gets sick. I've had a run in with salmonella and a ruptured appendix but the first was due to something I ate and the second was something that anyone could have! When my doc does my bloodwork, I have slightly higher than normal WBCs, and he says that is from all the T cells milling around because they aren't getting into my brain anymore. He says all it does is block T cells from crossing the blood/brain barrier and damaging myelin, and that it doesn't block all of them but enough are blocked to stop damage. I think that not enough is known to make a stand on what actually causes the JC virus to activate and cross the BBB. 80-85% of the population of the world carries the JC virus in their kidneys and it is usually dormant. PML has been seen in people with AIDS who are immune suppressed, in people who are treated with Rituxan, Tysabri, Raptiva, Cellcept, Methotrexate, Mitoxantrone, chemotherapeutic drugs, corticosteroids and some transplant drugs. Because of the PML cases associated with Tysabri, more has been learned about PML than ever before. It was previously known as a fatal disease. Now, with plasma exchange along with treatment with mefloquine or mirtazepine, and steroids if IRIS develops, people are living after diagnosis of PML. Reports on patients diagnosed with PML after Tysabri shows that most of the patients diagnosed so far are still alive. Some are doing well. Some of the earlier people are very disabled. The key seems to be increased vigilance and reporting ANY symptoms to your doctor. Since not many people are relapsing on Tysabri, when signs of relapse are seen, the new norm is to suspect PML first and vigorously test for it with blood tests, spinal taps, MRI, discontinuing Tysabri and further treatment if necessary. It COULD be just a relapse, but no one takes that chance now. Sorry to be so long-winded but you did ask...:p |
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If one were to look how first Betaseron, then Avonex, Copaxone and to a lesser extent Rebif, were tested and approved for MS, it is yet another classical story of how big pharma pushed these treatments into hugely revenue producing medications. But this is what happens when there was absolutely nothing to treat MS prior to these drugs showing up. Stats that were manipulated to show far better results than actually happened while the severe side effects were constantly minimized. It is not surprising at all that Tysabri has been embraced by many of those who use it because for the most part, the patient doesn't have to go through the bad side effects that many of you know all too well. It will be interesting to see what happens to Tysabri when the oral medications hit the market. And this will likely happen in the next couple of years. Harry |
RW: Thanks for all the useful information once again. Correct me if I'm wrong but AIDS the disease leads to the weakened immune system (low T cell count) not the drugs patients take. These patients don't take immunosuppressant drugs because that is counterintuitive and dangerous--hence, the effort to find antivirals that could wipe out or put into remission the HIV virus.
Just to add to what RW has said, while the idea of PML worries me, mostly when these cases arise, I am also planning to stay on Tysabri for the near future. I have been on it a year now and just recently I have noticed a big change in how I feel. It kind of snuck up on me. ALL my fatigue is now gone. I feel like I did before I got MS. I sometimes forget I have MS which is such a nice thing. It really is remarkable! :) I can see why people pushed for this drug to be offered again as an option. Anyhow, for now I am quite happy and feeling more assured that people are surviving PML and not all are seriously disabled. |
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I was in a rush and trying to get everything down before work and I got lost and didn't notice the error! :o I was thinking immune suppressed but I was ahead of it already trying to remember the names of the drugs associated with PML. |
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Cherie |
Tysabri works great for many of the people I know--which is about 10. The PML risk is there, and one should assume it fatal when it occcurs. The risk is higher for those who have received mutiple immune modulating therapies, especially when they have been given in close temporal proximity. If two immune modulating ("traditional") therapies fail to prevent flare ups then tysabri should be considered next along with other treatments--with the understanding of the risk of PML.
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